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连接到噬藻体 PBCV-1 主要衣壳蛋白的 N-连接寡糖的结构揭示了一类不寻常的复杂 N-聚糖。

Structure of N-linked oligosaccharides attached to chlorovirus PBCV-1 major capsid protein reveals unusual class of complex N-glycans.

机构信息

Department of Chemical Sciences, University of Napoli Federico II, 80126 Naples, Italy.

出版信息

Proc Natl Acad Sci U S A. 2013 Aug 20;110(34):13956-60. doi: 10.1073/pnas.1313005110. Epub 2013 Aug 5.

Abstract

The major capsid protein Vp54 from the prototype chlorovirus Paramecium bursaria chlorella virus 1 (PBCV-1) contains four Asn-linked glycans. The structure of the four N-linked oligosaccharides and the type of substitution at each glycosylation site was determined by chemical, spectroscopic, and spectrometric analyses. Vp54 glycosylation is unusual in many ways, including: (i) unlike most viruses, PBCV-1 encodes most, if not all, of the machinery to glycosylate its major capsid protein; (ii) the glycans are attached to the protein by a β-glucose linkage; (iii) the Asn-linked glycans are not located in a typical N-X-(T/S) consensus site; and (iv) the process probably occurs in the cytoplasm. The four glycoforms share a common core structure, and the differences are related to the nonstoichiometric presence of two monosaccharides. The most abundant glycoform consists of nine neutral monosaccharide residues, organized in a highly branched fashion. Among the most distinctive features of the glycoforms are (i) a dimethylated rhamnose as the capping residue of the main chain, (ii) a hyperbranched fucose unit, and (iii) two rhamnose residues with opposite absolute configurations. These glycoforms differ from what has been reported so far in the three domains of life. Considering that chloroviruses and other members of the family Phycodnaviridae may have a long evolutionary history, we suggest that the chlorovirus glycosylation pathway is ancient, possibly existing before the development of the endoplasmic reticulum and Golgi pathway, and involves still unexplored mechanisms.

摘要

原型绿藻噬藻体 Paramecium bursaria chlorella virus 1(PBCV-1)的主要衣壳蛋白 Vp54 含有四个 N-连接糖基化位点。通过化学、光谱和光谱分析确定了四个 N-连接寡糖的结构和每个糖基化位点的取代类型。Vp54 糖基化在许多方面都是不寻常的,包括:(i)与大多数病毒不同,PBCV-1 编码了大部分(如果不是全部)用于糖基化其主要衣壳蛋白的机制;(ii)糖基通过 β-葡萄糖键连接到蛋白质上;(iii)N-连接糖基化位点不在典型的 N-X-(T/S) 共识序列中;(iv)该过程可能发生在细胞质中。这四种糖型具有共同的核心结构,差异与两种单糖的非化学计量存在有关。最丰富的糖型由九个中性单糖残基组成,以高度支化的方式排列。糖型最显著的特征包括:(i)二甲基化鼠李糖作为主链的封端残基,(ii)超支化岩藻糖单元,以及(iii)两个具有相反绝对构型的鼠李糖残基。这些糖型与迄今为止在生命的三个领域中报道的糖型不同。考虑到噬藻体病毒和 Phycodnaviridae 科的其他成员可能具有悠久的进化历史,我们认为噬藻体病毒的糖基化途径是古老的,可能在内质网和高尔基体途径发展之前就存在,并且涉及尚未探索的机制。

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